Publications by authors named "Grant Hussey"

The human gut microbiome is a promising therapeutic target, but interventions are hampered by our limited understanding of microbial ecosystems. Here, we present a platform to develop, evaluate, and score approaches to learn ecological interactions from microbiome time series data. The microbiome time series inference standardized test (MTIST) comprises: a simulation framework for the generation of microbiome study data akin to what is obtained with quantitative next-generation sequencing approaches, a compilation of a large curated data set generated by the simulation framework representing 648 simulated microbiome studies containing 18,360 time series, with a total of 2,182,800 species abundance measurements, and a scoring method to rank ecological inference algorithms.

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Kinases are key players in cancer-relevant pathways and are the targets of many successful precision cancer therapies. Phosphoproteomics is a powerful approach to study kinase activity and has been used increasingly for the characterization of tumor samples leading to the identification of novel chemotherapeutic targets and biomarkers. Finding co-regulated phosphorylation sites which represent potential kinase-substrate sets or members of the same signaling pathway allows us to harness these data to identify clinically relevant and targetable alterations in signaling cascades.

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Longitudinal microbiome data provide valuable insight into disease states and clinical responses, but they are challenging to mine and view collectively. To address these limitations, we present TaxUMAP, a taxonomically informed visualization for displaying microbiome states in large clinical microbiome datasets. We used TaxUMAP to chart a microbiome atlas of 1,870 patients with cancer during therapy-induced perturbations.

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Article Synopsis
  • Gut microbiome dysbiosis is linked to COVID-19 severity, but a direct causal relationship has not been proven yet.
  • Research shows that SARS-CoV-2 infection leads to changes in gut bacteria in mice, which could compromise gut barrier function and increase infection risk.
  • Analysis of samples from 96 COVID-19 patients indicates that altered gut bacteria can enter the bloodstream, potentially causing severe secondary infections in these patients.
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Article Synopsis
  • * Research using a mouse model shows that SARS-CoV-2 infection disrupts the gut microbiome and affects gut cell function, mirroring findings in human patients.
  • * The study found that hospitalized COVID-19 patients have an overgrowth of harmful bacteria, including antibiotic-resistant strains, which are associated with secondary infections that may originate from the gut.
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Article Synopsis
  • The gut microbiome has been linked to the severity of COVID-19, but a direct causal relationship had not been clearly established before this study.
  • This research demonstrates that dysbiosis (imbalance) in the gut microbiome can lead to harmful bacteria entering the bloodstream during COVID-19, potentially causing serious infections.
  • Analysis of stool samples from COVID-19 patients showed significant microbiome imbalances, including an increase in harmful bacteria, which aligns with findings from a mouse model that confirms viral infection adversely affects gut health.
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Secondary active transporters couple the transport of an ion species down its concentration gradient to the uphill transport of another substrate. Despite the importance of secondary active transport to multidrug resistance, metabolite transport, and nutrient acquisition, among other biological processes, the microscopic steps of the coupling mechanism are not well understood. Often, transport models illustrate coupling mechanisms through a limited number of "major" conformations or states, yet recent studies have indicated that at least some transporters violate these models.

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The resistance of methicillin-resistant Staphylococcus aureus to antibiotics presents serious clinical problems that prompted the need for finding alternative or combination therapies. One such therapy is irradiation with blue light. To determine the alterations in metabolic processes implicated in the observed antimicrobial effects of blue light, we investigated the changes in membrane potential and the presence of free-radical-producing photo-acceptor molecules.

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